Your search keyword '"Wolfgang, Jungraithmayr"' showing total 4 results

1. Circulating Stromal Cell-Derived Factor 1α Levels in Heart Failure: A Matter of Proper Sampling.

Author

Lesley Baerts, Yannick Waumans, Inger Brandt, Wolfgang Jungraithmayr, Pieter Van der Veken, Marc Vanderheyden, and Ingrid De Meester

Subjects

Medicine, Science

Abstract

The chemokine Stromal cell-derived factor 1α (SDF1α, CXCL12) is currently under investigation as a biomarker for various cardiac diseases. The correct interpretation of SDF1α levels is complicated by the occurrence of truncated forms that possess an altered biological activity.We studied the immunoreactivities of SDF1α forms and evaluated the effect of adding a DPP4 inhibitor in sampling tubes on measured SDF1α levels. Using optimized sampling, we measured DPP4 activity and SDF1α levels in patients with varying degrees of heart failure.The immunoreactivities of SDF1α and its degradation products were determined with three immunoassays. A one hour incubation of SDF1α with DPP4 at 37°C resulted in 2/3 loss of immunoreactivity in each of the assays. Incubation with serum gave a similar result. Using appropriate sampling, SDF1α levels were found to be significantly higher in those heart failure patients with a severe loss of left ventricular function. DPP4 activity in serum was not altered in the heart failure population. However, the DPP4 activity was found to be significantly decreased in patients with high SDF1α levels.We propose that all samples for SDF1α analysis should be collected in the presence of at least a DPP4 inhibitor. In doing so, we found higher SDF1α levels in subgroups of patients with heart failure. Our work supports the need for further research on the clinical relevance of SDF1α levels in cardiac disease.

Published

2015

2. Chronic rejection pathology after orthotopic lung transplantation in mice: the development of a murine BOS model and its drawbacks.

Author

Stéphanie De Vleeschauwer, Wolfgang Jungraithmayr, Shana Wauters, Stijn Willems, Manuela Rinaldi, Annemie Vaneylen, Stijn Verleden, Anna Willems-Widyastuti, Ken Bracke, Guy Brusselle, Erik Verbeken, Dirk Van Raemdonck, Geert Verleden, and Bart Vanaudenaerde

Subjects

Medicine, Science

Abstract

Almost all animal models for chronic rejection (CR) after lung transplantation (LTx) fail to resemble the human situation. It was our attempt to develop a representative model of CR in mice. Orthotopic LTx was performed in allografts receiving daily immunosuppression with steroids and cyclosporine. Controls included isografts and mice only undergoing thoracotomy (SHAM). Allografts were sacrificed 2, 4, 6, 8, 10 or 12 weeks after LTx. Pulmonary function was measured repeatedly in the 12w allografts, isografts and SHAM mice. Histologically, all allografts demonstrated acute rejection (AR) around the blood vessels and airways two weeks after LTx. This decreased to 50-75% up to 10 weeks and was absent after 12 weeks. Obliterative bronchiolitis (OB) lesions were observed in 25-50% of the mice from 4-12 weeks. Isografts and lungs of SHAM mice were normal after 12 weeks. Pulmonary function measurements showed a decline in FEV(0.1), TLC and compliance in the allografts postoperatively (2 weeks) with a slow recovery over time. After this initial decline, lung function of allografts increased more than in isografts and SHAM mice indicating that pulmonary function measurement is not a good tool to diagnose CR in a mouse. We conclude that a true model for CR, with clear OB lesions in about one third of the animals, but without a decline in lung function, is possible. This model is an important step forward in the development of an ideal model for CR which will open new perspectives in unraveling CR pathogenesis and exploring new treatment options.

Published

2012

3. Chronic rejection pathology after orthotopic lung transplantation in mice : the development of a murine BOS model and its drawbacks

Author

Stijn E. Verleden, Dirk Van Raemdonck, Ken R. Bracke, Geert Verleden, Annemie Vaneylen, Manuela Rinaldi, Shana Wauters, Wolfgang Jungraithmayr, Stéphanie De Vleeschauwer, Erik Verbeken, Anna Willems-Widyastuti, Guy Brusselle, Bart M. Vanaudenaerde, Stijn Willems, and Gregson, Aric

Subjects

Graft Rejection, Male, Pathology, Time Factors, Pulmonology, medicine.medical_treatment, Injury, OBLITERATIVE BRONCHIOLITIS, Pulmonary function testing, Pathogenesis, Mice, Allograft, ANIMAL-MODEL, Medicine and Health Sciences, Thoracotomy, Bronchiolitis Obliterans, Mice, Inbred BALB C, Multidisciplinary, Immunosuppression, MOUSE MODEL, Animal Models, Syndrome, Medicine, Engineering sciences. Technology, Research Article, Lung Transplantation, medicine.medical_specialty, Animal-Model, Clinical Research Design, Science, Immunology, Bronchiolitis obliterans, ALLOGRAFT, Model Organisms, Diagnostic Medicine, INJURY, medicine, Lung transplantation, Animals, Humans, Transplantation, Homologous, Biology, Mouse Model, business.industry, Histology, Immunologic Subspecialties, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, Bronchiolitis, Anatomical Pathology, Chronic Disease, Clinical Immunology, Surgery, business, Obliterative Bronchiolitis

Abstract

Almost all animal models for chronic rejection (CR) after lung transplantation (LTx) fail to resemble the human situation. It was our attempt to develop a representative model of CR in mice. Orthotopic LTx was performed in allografts receiving daily immunosuppression with steroids and cyclosporine. Controls included isografts and mice only undergoing thoracotomy (SHAM). Allografts were sacrificed 2, 4, 6, 8, 10 or 12 weeks after LTx. Pulmonary function was measured repeatedly in the 12w allografts, isografts and SHAM mice. Histologically, all allografts demonstrated acute rejection (AR) around the blood vessels and airways two weeks after LTx. This decreased to 50-75% up to 10 weeks and was absent after 12 weeks. Obliterative bronchiolitis (OB) lesions were observed in 25-50% of the mice from 4-12 weeks. Isografts and lungs of SHAM mice were normal after 12 weeks. Pulmonary function measurements showed a decline in FEV0.1, TLC and compliance in the allografts postoperatively (2 weeks) with a slow recovery over time. After this initial decline, lung function of allografts increased more than in isografts and SHAM mice indicating that pulmonary function measurement is not a good tool to diagnose CR in a mouse. We conclude that a true model for CR, with clear OB lesions in about one third of the animals, but without a decline in lung function, is possible. This model is an important step forward in the development of an ideal model for CR which will open new perspectives in unraveling CR pathogenesis and exploring new treatment options. GV is holder of the GSK (Belgium) chair in respiratory pharmacology at the Katholieke Universiteit Leuven (KUL), and is supported by grants from the KUL (OT/050/10) and the FWO (Fonds Wetenschappelijk Onderzoek)-Flanders: G.0643.08 and G.0723.10. DVR and BV are senior clinical investigators of the FWOFlanders. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript

Published

2012

4. Circulating Stromal Cell-Derived Factor 1α Levels in Heart Failure: A Matter of Proper Sampling

Author

Yannick Waumans, Ingrid De Meester, Inger Brandt, Pieter Van der Veken, Lesley Baerts, Wolfgang Jungraithmayr, and Marc Vanderheyden

Subjects

medicine.medical_specialty, Dipeptidyl Peptidase 4, Population, lcsh:Medicine, Hemodynamics, Biology, Internal medicine, medicine, Humans, Clinical significance, lcsh:Science, education, Incubation, Aged, Heart Failure, Immunoassay, Dipeptidyl-Peptidase IV Inhibitors, education.field_of_study, Multidisciplinary, Ejection fraction, Pharmacology. Therapy, lcsh:R, Biological activity, medicine.disease, Chemokine CXCL12, Endocrinology, Heart failure, Proteolysis, Biomarker (medicine), lcsh:Q, Human medicine, Engineering sciences. Technology, Blood Chemical Analysis, Research Article

Abstract

Background The chemokine Stromal cell-derived factor 1α (SDF1α, CXCL12) is currently under investigation as a biomarker for various cardiac diseases. The correct interpretation of SDF1α levels is complicated by the occurrence of truncated forms that possess an altered biological activity. Methodology We studied the immunoreactivities of SDF1α forms and evaluated the effect of adding a DPP4 inhibitor in sampling tubes on measured SDF1α levels. Using optimized sampling, we measured DPP4 activity and SDF1α levels in patients with varying degrees of heart failure. Results The immunoreactivities of SDF1α and its degradation products were determined with three immunoassays. A one hour incubation of SDF1α with DPP4 at 37°C resulted in 2/3 loss of immunoreactivity in each of the assays. Incubation with serum gave a similar result. Using appropriate sampling, SDF1α levels were found to be significantly higher in those heart failure patients with a severe loss of left ventricular function. DPP4 activity in serum was not altered in the heart failure population. However, the DPP4 activity was found to be significantly decreased in patients with high SDF1α levels Conclusions We propose that all samples for SDF1α analysis should be collected in the presence of at least a DPP4 inhibitor. In doing so, we found higher SDF1α levels in subgroups of patients with heart failure. Our work supports the need for further research on the clinical relevance of SDF1α levels in cardiac disease.

Published

2015